Published on: 10 Jul 2014 CRISANTA LS Tablets (Drospirenone + Ethinylestradiol) Black Box Warning Cigarette Smoking and Serious Cardiovoscular Events: Cigarette smoking increases the risk of serious cardiovascular events from combination oral contraceptives (COC) use. This risk increases with age, particularly in women over 35 years of age and with the number of cigarettes smoked. For this reason, COCs should not be used by women who are over 35 years of age and smoke. Composition Each film-coated tablet contains: Drospirenone. 3 mg Ethinylestradiol. 0.02 mg Dosage Form Tablets for oral use. Description CRISANTA-LS an oral contraceptive. Each pack consists of 24 tablets, and each tablet contains 3 mg of drospirenone (DRSP) and 0.02 mg of ethinylestradiol (EE). Pharmacology Pharmacodynamics Drospirenone is a spironolactone analogue with anti-mineralocorticoid and anti-androgenic activity. The oestrogen in CRISANTA-LS is ethinylestradiol. COCs lower the risk of becoming pregnant primarily by suppressing ovulation. Other possible mechanisms may include cervical mucus changes that inhibit sperm penetration and the endometrial changes that reduce the likelihood of implantation. Acne Acne vulgaris is a skin condition with a multifactorial aetiology, including androgen stimulation of sebum production. While the combination of EE and DRSP increases sex hormone-binding globulin (SHBG) and decreases free testosterone, the relationship between these changes and a decrease in the severity of facial acne in otherwise healthy women with this skin condition has not been established. The impact of the anti-androgenic activity of DRSP on acne is not known. Pharmacokinetics Absorption
The absolute bioavailability of DRSP from a single entity tablet is about 76%. The absolute bioavailability of EE is approximately 40% as a result of presystemic conjugation and first-pass metabolism. Serum concentrations of DRSP and EE reached peak levels within 1-2 hours after the administration. The pharmacokinetics of DRSP is dose proportional following single doses ranging from 1-10 mg. Following daily dosing of DRSP and EE, steady-state DRSP concentrations were observed after 8 days. There was about 2-3 fold accumulation in serum C max and AUC (0-24h) values of DRSP following multiple-dose administration of DRSP and EE. For EE, steady-state conditions are reported during the second half of a treatment cycle. Following daily administration of DRSP and EE, serum C max and AUC (0 24h) values of EE accumulate by a factor of about 1.5-2. Pharmacokinetic Parameters of DRSP and EE DRSP 1 2 1 Cycle/day No. of subjects C max (ng/ml) T max (h) AUC (0-24h)1 (ng h/ml) t 1/2 (h) 1/1 23 38.4 (25) 1.5 (1-2) 1/21 23 70.3 (15) 1.5 (1-2) 268 (19) NA 763 (17) 30.8 (22) EE Cycle/day No. of subjects C max 1 (pg/ml) T max 2 (h) AUC (0-24h)1 (pg h/ml) t 1/2 1 (h) 1/1 23 32.8 (45) 1.5 (1-2) 1/21 23 45.1 (35) 1.5 (1-2) 108 (52) NA 220 (57) NA NA = Not available 1 : geometric mean (geometric coefficient of variation) 2 : median (range) Effect of Food The rate of absorption of DRSP and EE following single administration of a formulation similar to DRSP and EE was slower under fed (high fat meal) conditions with the serum C max being reduced about 40% for both components. The extent of absorption of DRSP, however, remained unchanged. In contrast, the extent of absorption of EE was reduced by about 20% under fed conditions. Distribution DRSP and EE serum concentrations decline in two phases. The apparent volume of distribution of DRSP is approximately 4 L/kg and that of EE is reported to be approximately 4-5 L/kg. DRSP does not bind to SHBG or corticosteroid binding globulin (CBG) but binds about 97% to other serum proteins. Multiple dosing over 3 cycles resulted in no change in the free fraction (as measured at trough concentrations). EE is reported to be highly but non-specifically bound to serum albumin (approximately 98.5%) and induces an increase in the serum concentrations of both SHBG and CBG. EE induced effects on SHBG and CBG were not affected by variation of the DRSP dosage in the range of 2-3 mg. Metabolism The two main metabolites of DRSP found in human plasma were identified to be the acid form of DRSP generated by
opening of the lactone ring and the 4, 5-dihydrodrospirenone-3-sulphate. These metabolites were shown not to be pharmacologically active. In in vitro studies with human liver microsomes, DRSP was metabolized only to a minor extent mainly by CYP3A4. EE has been reported to be subject to presystemic conjugation in both small bowel mucosa and the liver. Metabolism occurs primarily by aromatic hydroxylation but a wide variety of hydroxylated and methylated metabolites are formed. These are present as free metabolites and as conjugates with glucuronide and sulphate. CYP3A4 in the liver is responsible for the 2-hydroxylation which is the major oxidative reaction. The 2-hydroxy metabolite is further transformed by methylation and glucuronidation prior to urinary and faecal excretion. Excretion DRSP serum concentrations are characterized by a terminal disposition phase half-life of approximately 30 hours after both single- and multiple- dose regimens. Excretion of DRSP was nearly complete after 10 days and amounts excreted were slightly higher in faeces compared with urine. DRSP was extensively metabolized and only trace amounts of unchanged DRSP were excreted in urine and faeces. At least 20 different metabolites were observed in urine and faeces. About 38-47% of the metabolites in urine were glucuronide and sulphate conjugates. In faeces, about 17-20% of the metabolites were excreted as glucuronides and sulphates. For EE the terminal disposition phase half-life has been reported to be approximately 24 hours. EE is not excreted unchanged. EE is excreted in the urine and faeces as glucuronide and sulphate conjugates and undergoes enterohepatic circulation. Special Populations Renal Impairment DRSP+EE is contraindicated in patients with renal impairment. In subjects with creatinine clearance (CLcr) of 50-79 ml/min, serum DRSP levels were comparable to those in a control group with CLcr > 80 ml/min. In subjects with serum DRSP concentrations were on average 37% higher than those in the control group. In addition, there is a potential to develop hyperkalaemia in subjects with renal impairment whose serum potassium is in the upper reference range, and who are concomitantly using potassium sparing drugs. Hepatic Impairment DRSP+EE is contraindicated in patients with hepatic disease. The mean exposure to DRSP in women with moderate liver impairment is approximately three times higher than the exposure in women with normal liver function. DRSP and EE have not been studied in women with severe hepatic impairment. Paediatric Population Safety and efficacy of DRSP+EE has been established in women of reproductive age. Efficacy is expected to be the same for postpubertal adolescents under the age of 18 and for users 18 years and older. Use of this product before menarche is not indicated. Geriatric Population DRSP+EE has not been studied in postmenopausal women and is not indicated in this population. Indications CRISANTA-LS is indicated for: Use by women to prevent pregnancy. Treatment of moderate acne vulgaris in women at least 14 years of age, who have no known contraindications to oral contraceptive therapy and have achieved menarche. CRISANTA-LS should be used for the treatment of acne only if the patient desires an oral contraceptive for birth control.
Treatment of symptoms of premenstrual dysphoric disorder (PMDD) in women who choose to use an oral contraceptive as their method of contraception. The effectiveness of CRISANTA-LS for PMDD when used for more than three menstrual cycles has not been evaluated. Dosage And Administration CRISANTA-LS consists of 24 tablets of a monophasic combined hormonal preparation. The dosage of CRISANTA-LS is one tablet daily for 24 consecutive days followed by 4 pill-free days per menstrual cycle. How to take CRISANTA-LS Take one tablet by mouth at the same time every day. The failure rate may increase when pills are missed or taken incorrectly. To achieve maximum effectiveness, CRISANTA-LS must be taken exactly as directed, in the order directed on the pack. Single missed pills should be taken as soon as remembered. How to Start CRISANTA-LS During the first cycle of CRISANTA-LS use, instruct the patient to take one tablet of CRISANTA-LS daily, beginning on Day 1 of her menstrual cycle (the first day of menstruation is Day 1). She should take one tablet daily for 24 consecutive days followed by 4 pill-free days. CRISANTA-LS should be taken in the order directed on the package at the same time each day, preferably after the evening meal or at bedtime with some liquid, as needed. CRISANTA-LS can be taken without regard to meals. If CRISANTA-LS is first taken later than the first day of the menstrual cycle, it should not be considered effective as a contraceptive until after the first 7 consecutive days of product administration. Instruct the patient to use a non-hormonal contraceptive as back-up during the first 7 days. The possibility of ovulation and conception prior to initiation of medication should be considered. Instructions for Patients
Subsequent Packs of CRISANTA-LS The patient should begin her next and all subsequent 24-day regimens of CRISANTA-LS on the same day of the week that she began her first regimen, following the same schedule. She should begin taking her tablets on the next day after the 4 pill-free days, regardless of whether or not a menstrual period has occurred or is still in progress. Anytime a subsequent cycle of CRISANTA-LS is started later than the day following the 4 pill-free days, the patient should use another method of contraception until she has taken CRISANTA-LS daily for 7 consecutive days. Switching When Switching From a Different Birth Control Pill When switching from another birth control pill, CRISANTA-LS should be started on the same day that a new pack of the previous oral contraceptive would have been started. When Switching From a Method other than a Birth Control Pill When switching from a transdermal patch or vaginal ring, CRISANTA-LS should be started preferably on the day of removal, but at the latest when the next application would have been due. When switching from an injection, CRISANTA-LS should be started when the next dose would have been due. When switching from an intrauterine contraceptive or an implant, CRISANTA-LS should be started on the day of removal. The woman should, in all of these cases, be advised to additionally use a barrier method for the first 7 days of tablettaking. Withdrawal bleeding usually occurs within 3 days following the last tablet. If spotting or breakthrough bleeding occurs while taking CRISANTA-LS, instruct the patient to continue taking CRISANTA-LS as per the regimen described above. Counsel her that this type of bleeding is usually transient and without significance; however, if the bleeding is persistent or prolonged, she should consult her physician. Following first-trimester abortion, the woman may start CRISANTA-LS immediately. When doing so, she need not take additional contraceptive measures. For postpartum women who do not breastfeed or after a second trimester abortion, start CRISANTA-LS no earlier than 4 weeks postpartum due to the increased risk of thromboembolism. If the patient starts on CRISANTA-LS postpartum and has not yet had a period, evaluate for possible pregnancy, and instruct her to use an additional method of contraception until she has taken CRISANTA-LS for 7 consecutive days. Although the occurrence of pregnancy is low if CRISANTA-LS is taken according to directions, if withdrawal bleeding does not occur, the possibility of pregnancy must be considered. If the patient has not adhered to the prescribed dosing schedule (missed one or more tablets or started taking them on a day later than she should have), the possibility of pregnancy should be considered at the time of the first missed period and appropriate diagnostic measures taken. If the patient has adhered to the prescribed regimen and misses two consecutive periods, pregnancy should be ruled out. Hormonal contraceptives should be discontinued if pregnancy is confirmed. The risk of pregnancy increases with each tablet missed. If breakthrough bleeding occurs following missed tablets, it will usually be transient and of no consequence. Missed Pill The risk of pregnancy increases with each tablet missed. If she MISSES one tablet: Ask her to take it as soon as she remembers. Ask her to take the next tablet at her regular time. This means she may take two tablets in one day. She does not need to use a back-up birth control method if she has sex. If she MISSES two tablets in a row in WEEK 1 OR WEEK 2 of the pack:
Ask her to take two tablets on the day she remembers and two tablets the next day. Then ask her to take one tablet a day until she finishes the pack. She could become pregnant if she has sex in the 7 days after she restarts her tablets. She must use another birth control method (such as condoms or spermicides) as a back-up for those 7 days. If she MISSES two tablets in a row in WEEK 3 or Week 4 of the pack: Ask her to throw out the rest of the pack and start a new pack that same day. She could become pregnant if she has sex in the 7 days after she restarts her tablets. She must use another birth control method (such as condoms or spermicides) as a back-up for those 7 days. She may not have her period this month but this is expected. However, if she misses her period 2 months in a row, ask her to contact her doctor or clinic because she might be pregnant. If she MISSES three OR more tablets in a row during ANY Week: Ask her to throw out the rest of the pack and start a new pack that same day. She could become pregnant if she has sex in the 7 days after she restarts her tablets. She must use another birth control method (such as condoms or spermicides) as a back-up for those 7 days. She may not have her period this month but this is expected. However, if she misses her period 2 months in a row, ask her to contact her doctor or clinic because she might be pregnant. Finally, if she is still not sure what to do about the tablets she has missed: Ask her to use a back-up method (such as condoms or spermicides) anytime she has sex. Ask her to continue taking 1 tablet each day until she contacts her doctor. Advice in Case of Gastrointestinal Disturbances In case of severe vomiting or diarrhoea, absorption may not be complete and additional contraceptive measures should be taken. If vomiting occurs within 3 4 hours after tablet-taking, this can be regarded as a missed tablet. Contraindications DRSP+EE should not be used in women who have the following: Renal impairment Adrenal insufficiency A high risk of arterial or venous thrombotic diseases. Examples include women who are known to: Smoke, if over age 35 Have deep vein thrombosis or pulmonary embolism, now or in the past Have cerebrovascular disease Have coronary artery disease Have thrombogenic valvular or thrombogenic rhythm diseases of the heart (e.g., subacute bacterial endocarditis with valvular disease, or atrial fibrillation) Have inherited or acquired hypercoagulopathies Have uncontrolled hypertension Have diabetes mellitus with vascular disease Have headaches with focal neurological symptoms or have migraine headaches with or without aura if over age 35 Undiagnosed abnormal uterine bleeding Breast cancer or other oestrogen- or progestin-sensitive cancer, now or in the past Liver tumours, benign or malignant, or liver disease Pregnancy, because there is no reason to use COCs during pregnancy
Hypersensitivity to any component of this product Warnings And Precautions General Thromboembolic Disorders and Other Vascular Problems Stop DRSP+EE if an arterial or venous thrombotic (VTE) event occurs. Based on presently available information on DRSP-containing COCs with 0.03 mg EE, DRSP containing COCs may be associated with a higher risk of VTE than COCs containing the progestin levonorgestrel or some other progestins. Epidemiologic studies that compared the risk of VTE reported that the risk ranged from no increase to a 3-fold increase. Before initiating use of DRSP+EE in a new COC user or a woman who is switching from a contraceptive that does not contain DRSP, consider the risks and benefits of a DRSP-containing COC in light of her risk for a VTE. Known risk factors for VTE include smoking, obesity, and family history of VTE, in addition to other factors that contraindicate use of COCs. Although the absolute VTE rates are increased for users of hormonal contraceptives compared to non-pregnant, nonusers (1-5 per 10,000 woman-years), the rates during pregnancy (5-20 per 10,000 woman-years) are even greater, especially during the postpartum period (40-65 per 10,000 woman-years). The risk of VTE in women using COCs has been estimated to be 3-9 per 10,000 woman-years. The risk of VTE is highest during the first year of use. Data from a large, prospective cohort safety study of various COCs suggest that this increased risk, as compared with that in non- COC users, is greatest during the first 6 months of COC use. Data from this safety study indicate that the greatest risk of VTE is present after initially starting a COC or restarting (following a 4-week or greater pill-free interval) the same or a different COC. The risk of thromboembolic disease due to oral contraceptives gradually disappears after COC use is discontinued. If feasible, stop DRSP+EE at least 4 weeks before and through 2 weeks after major surgery or other surgeries known to have an elevated risk of thromboembolism. Start DRSP+EE no earlier than 4 weeks after delivery, in women who are not breastfeeding. The risk of postpartum thromboembolism decreases after the third postpartum week, whereas the risk of ovulation increases after the third postpartum week. Use of COCs also increases the risk of arterial thromboses such as strokes and myocardial infarctions, especially in women with other risk factors for these events. COCs have been shown to increase both the relative and attributable risks of cerebrovascular events (thrombotic and haemorrhagic strokes), although, in general, the risk is greatest among older (>35 years of age), hypertensive women who also smoke. COCs also increase the risk for stroke in women with other underlying risk factors. Oral contraceptives must be used with caution in women with cardiovascular disease risk factors. Stop DRSP+EE if there is unexplained loss of vision, proptosis, diplopia, papilledema, or retinal vascular lesions. Evaluate for retinal vein thrombosis immediately. Hyperkalaemia The progestin DRSP has anti-mineralocorticoid activity, including the potential for hyperkalaemia in high risk patients, comparable with a 25 mg dose of spironolactone. DRSP+EE should not be used in patients with conditions that predispose to hyperkalaemia (i.e. renal impairment, hepatic impairment and adrenal insufficiency). Women receiving daily, long-term treatment for chronic conditions or diseases with medications that may increase serum potassium concentration should have their serum potassium concentration checked during the first treatment cycle. Medications that may increase serum potassium concentration include ace inhibitors, angiotensin-ii receptor antagonists, potassiumsparing diuretics, potassium supplementation, heparin, aldosterone antagonists and NSAIDs. Consider monitoring serum
potassium concentration in high-risk patients who take a strong CYP3A4 inhibitor long-term and concomitantly. Strong CYP3A4 inhibitors include azole antifungals (e.g. ketoconazole, itraconazole, voriconazole), HIV/HCV protease inhibitors (e.g. indinavir, boceprevir), and clarithromycin. Carcinoma of the Breasts and Reproductive Organs Women who currently have or have had breast cancer should not use DRSP+EE because breast cancer is a hormonallysensitive tumour. There is substantial evidence that COCs do not increase the incidence of breast cancer. Although some past studies have suggested that COCs might increase the incidence of breast cancer, more recent studies have not confirmed such findings. Some studies suggest that COCs are associated with an increase in the risk of cervical cancer or intraepithelial neoplasia. However, there is controversy about the extent to which these findings may be due to differences in sexual behaviour and other factors. Liver Disease Discontinue DRSP+EE if jaundice develops. Steroid hormones may be poorly metabolized in patients with impaired liver function. Acute or chronic disturbances of liver function may necessitate the discontinuation of COC use until markers of liver function return to normal and COC causation has been excluded. Hepatic adenomas are associated with COC use. An estimate of the attributable risk is 3.3 cases/100,000 COC users. Rupture of hepatic adenomas may cause death through intra-abdominal haemorrhage. Studies have shown an increased risk of developing hepatocellular carcinoma in long-term (>8 years) COC users. However, the attributable risk of liver cancers in COC users is less than one case per million users. Oral contraceptive-related cholestasis may occur in women with a history of pregnancy-related cholestasis. Women with a history of COC-related cholestasis may have the condition recur with subsequent COC use. High Blood Pressure For women with well-controlled hypertension, monitor blood pressure and stop DRSP+EE if blood pressure rises significantly. Women with uncontrolled hypertension or hypertension with vascular disease should not use COCs. An increase in blood pressure has been reported in women taking COCs, and this increase is more likely in older women and with extended duration of use. The incidence of hypertension increases with increasing concentration of progestin. Gallbladder Disease Studies suggest a small increased relative risk of developing gallbladder disease among COC users. Carbohydrate and Lipid Metabolic Effects Carefully monitor prediabetic and diabetic women who are taking DRSP+EE. COCs may decrease glucose intolerance in a dose-related fashion. Consider alternative contraception for women with uncontrolled dyslipidaemias. A small proportion of women will have adverse lipid changes while on COCs. Women with hypertriglyceridaemia, or a family history thereof, may be at an increased risk of pancreatitis when using COCs. Headache If a woman taking DRSP+EE develops new headaches that are recurrent, persistent, or severe, evaluate the cause and discontinue DRSP+EE if indicated. An increase in frequency or severity of migraine during COC use (which may be prodromal of a cerebrovascular event) may be a reason for immediate discontinuation of the COC. Bleeding Irregularities Unscheduled (breakthrough or intracyclic) bleeding and spotting sometimes occur in patients on COCs, especially during the first 3 months of use. If bleeding persists or occurs after previously regular cycles, check for causes such as pregnancy or malignancy. If pathology and pregnancy are excluded, bleeding irregularities may resolve over time or with a change to a different COC. Women who use DRSP+EE may experience absence of withdrawal bleeding, even if they are not pregnant. Some women may encounter post-pill amenorrhoea or oligomenorrhoea, especially when such a condition was pre-existent. If withdrawal bleeding does not occur, consider the possibility of pregnancy. If the patient has not adhered to the prescribed dosing schedule (missed one or more active tablets or started taking
them on a day later than she should have), consider the possibility of pregnancy at the time of the first missed period and take appropriate diagnostic measures. If the patient has adhered to the prescribed regimen and misses two consecutive periods, rule out pregnancy. COC Use Before or During Early Pregnancy Extensive epidemiological studies have revealed no increased risk of birth defects in women who have used oral contraceptives prior to pregnancy. Studies also do not suggest a teratogenic effect, particularly in so far as cardiac anomalies and limb-reduction defects are concerned, when taken inadvertently during early pregnancy. The administration of oral contraceptives to induce withdrawal bleeding should not be used as a test for pregnancy. Depression Women with a history of depression should be carefully observed and DRSP+EE discontinued if depression recurs to a serious degree. Interference with Laboratory Tests The use of COCs may change the results of some laboratory tests, such as coagulation factors, lipids, glucose tolerance, and binding proteins. Women on thyroid hormone replacement therapy may need increased doses of thyroid hormone because serum concentrations of thyroid-binding globulin increase with use of COCs. DRSP causes an increase in plasma renin activity and plasma aldosterone induced by its mild anti-mineralocorticoid activity. Monitoring A woman who is taking COCs should have a yearly visit with her healthcare provider for a blood pressure check and for other indicated healthcare. Other Conditions In women with hereditary angio-oedema, exogenous oestrogens may induce or exacerbate symptoms of angio-oedema. Chloasma may occasionally occur, especially in women with a history of chloasma gravidarum. Women with a tendency to chloasma should avoid exposure to the sun or ultraviolet radiation while taking COCs. Lactose Intolerance Each tablet of this medicinal product contains lactose. Patients with rare hereditary problems of galactose intolerance, the Lapp lactase deficiency, or glucose-galactose malabsorption should not take this medicine. Drug Interactions Consult the labelling of all concurrently-used drugs to obtain further information about interactions with hormonal contraceptives or the potential for enzyme alterations. Effects of Other Drugs on Combined Hormonal Contraceptives Substances Diminishing the Efficacy of COCs Drugs or herbal products that induce certain enzymes, including CYP3A4, may decrease the effectiveness of COCs or increase breakthrough bleeding. Some drugs or herbal products that may decrease the effectiveness of hormonal contraceptives include phenytoin, barbiturates, carbamazepine, bosentan, felbamate, griseofulvin, oxcarbazepine, rifampicin, topiramate and products containing St. John s wort. Interactions between oral contraceptives and other drugs may lead to breakthrough bleeding and/or contraceptive failure. Counsel women to use an alternative method of contraception or a back-up method when enzyme inducers are used with COCs, and to continue back-up contraception for 28 days after discontinuing the enzyme inducer to ensure contraceptive reliability. Substances Increasing the Plasma Concentrations of COCs Co-administration of atorvastatin and certain COCs containing EE increase AUC values for EE by approximately 20%. Ascorbic acid andacetaminophen may increase plasma EE concentrations, possibly by inhibition of conjugation. Concomitant administration of moderate or strong CYP3A4 inhibitors such as azole antifungals (e.g. ketoconazole, itraconazole, voriconazole, fluconazole), verapamil, macrolides (e.g. clarithromycin, erythromycin), diltiazem, and
grapefruit juice can increase the plasma concentrations of the oestrogen or the progestin or both. Human Immunodeficiency Virus (HIV)/ Hepatitis C Virus (HCV) Protease Inhibitors and Non-nucleoside Reverse Transcriptase Inhibitors Significant changes (increase or decrease) in the plasma concentrations of oestrogen and progestin have been noted in some cases of co-administration with HIV/HCV protease inhibitors or with non-nucleoside reverse transcriptase inhibitors. Antibiotics There have been reports of pregnancy while taking hormonal contraceptives and antibiotics, but clinical pharmacokinetic studies have not shown consistent effects of antibiotics on plasma concentrations of synthetic steroids. Effect on DRSP The main metabolites of DRSP in human plasma are generated without involvement of the CYP system. Inhibitors of this enzyme system are, therefore, unlikely to influence the metabolism of DRSP. Effects of COCs on Other Drugs COCs containing EE may inhibit the metabolism of other compounds. COCs have been shown to significantly decrease plasma concentrations of lamotrigine, likely due to induction of lamotrigine glucuronidation. This may reduce seizure control; therefore, dosage adjustments of lamotrigine may be necessary. Consult the labelling of the concurrently-used drug to obtain further information about interactions with COCs or the potential for enzyme alterations. In vitro and clinical studies did not indicate an inhibitory potential of DRSP towards human CYP enzymes at clinically relevant concentrations. Women on thyroid hormone replacement therapy may need increased doses of thyroid hormone because serum concentration of thyroid-binding globulin increases with use of COCs. Potential to Increase Serum Potassium Concentration There is a potential for an increase in serum potassium concentration in women taking DRSP+EE with other drugs that may increase serum potassium concentration. Interference with Laboratory Tests The use of contraceptive steroids may influence the results of certain laboratory tests, such as coagulation factors, lipids, glucose tolerance, and binding proteins. DRSP causes an increase in plasma renin activity and plasma aldosterone induced by its mild anti-mineralocorticoid activity. Renal Impairment DRSP+EE is contraindicated in patients with renal impairment. Hepatic Impairment DRSP+EE is contraindicated in patients with hepatic disease. Pregnancy Pregnancy Category X DRSP+EE is contraindicated during pregnancy. There is little or no increased risk of birth defects in women who inadvertently use COCs during early pregnancy. Epidemiologic studies and meta-analyses have not found an increased risk of genital or non-genital birth defects (including cardiac anomalies and limb-reduction defects) following exposure to low dose COCs prior to conception or during early pregnancy. The administration of COCs to induce withdrawal bleeding should not be used as a test for pregnancy. COCs should not be used during pregnancy to treat threatened or habitual abortion. Women who do not breastfeed may start COCs no earlier than 4 weeks postpartum.
Lactation When possible, advise the nursing mother to use other forms of contraception until she has weaned her child. Oestrogen-containing COCs can reduce milk production in breastfeeding mothers. This is less likely to occur once breastfeeding is well-established; however, it can occur at any time in some women. Small amounts of oral contraceptive steroids and/or metabolites are present in breast milk. After oral administration of 3 mg DRSP/0.03 mg EE tablets, about 0.02% of the DRSP dose was excreted into the breast milk of postpartum women within 24 hours. This results in a maximal daily dose of about 0.003 mg DRSP in an infant. Paediatric Use Safety and efficacy of DRSP+EE has been established in women of reproductive age. Efficacy is expected to be the same for postpubertal adolescents under the age of 18 years and for users aged 18 years and older. Use of this product before menarche is not indicated. Geriatric Use DRSP+EE has not been studied in postmenopausal women and is not indicated in this population. Undesirable Effects The following serious adverse reactions with the use of COCs are discussed elsewhere in the labelling: Serious cardiovascular events and stroke Vascular events Liver disease Adverse reactions commonly reported by COC users are: Irregular uterine bleeding Nausea Breast tenderness Headache Clinical Trials Experience Because clinical trials are conducted under widely varying conditions, adverse reaction rates observed in the clinical trials of a drug cannot be directly compared with rates in the clinical trials of another drug and may not reflect the rates observed in practice. Contraception and Acne Clinical Trials The data provided reflect the experience with the use of DRSP and EE in the adequate and well-controlled studies for contraception (N=1,056) and for moderate acne vulgaris (N=536). The adverse reactions seen across the two indications overlapped, and are reported using the frequencies from the pooled dataset. The most common adverse reactions (> 2% of users) were: Headache/migraine (6.7%), menstrual irregularities (including vaginal haemorrhage and metrorrhagia (4.7%), nausea/vomiting (4.2%), breast pain/tenderness (4%) and mood changes (2.2%). Premenstrual Dysphoric Disorder (PMDD) Clinical Trials Safety data from trials for the indication of PMDD are reported separately due to differences in study design and setting in the Contraception and Acne studies as compared with the PMDD clinical program. Common adverse reactions (> 2% of users) were: Menstrual irregularities (including vaginal haemorrhage and metrorrhagia) (24.9%), nausea (15.8%), headache (13.0%), breast tenderness (10.5%), fatigue (4.2%), irritability (2.8%), decreased libido (2.8%), increased weight (2.5%), and affect lability (2.1%).
Adverse Reactions (> 1%) Leading to Study Discontinuation Contraception Clinical Trials Of 1,056 women, 6.6% discontinued from the clinical trials due to an adverse reaction; the most frequent adverse reactions leading to discontinuation were headache/migraine (1.6%) and nausea/vomiting (1.0%). Acne Clinical Trials Of 536 women, 5.4% discontinued from the clinical trials due to an adverse reaction; the most frequent adverse reaction leading to discontinuation was menstrual irregularities (including menometrorrhagia, menorrhagia, metrorrhagia and vaginal haemorrhage; 2.2%). PMDD Clinical Trials Of 285 women, 11.6% discontinued from the clinical trials due to an adverse reaction; the most frequent adverse reactions leading to discontinuation were: nausea/vomiting (4.6%), menstrual irregularity (including vaginal haemorrhage, menorrhagia, menstrual disorder, menstruation irregular and metrorrhagia; 4.2%), fatigue (1.8%), breast tenderness (1.4%), depression (1.4%), headache (1.1%), and irritability (1.1%). Serious Adverse Reactions Contraception Clinical Trials: migraine and cervical dysplasia Acne Clinical Trials: none reported in the clinical trials PMDD Clinical Trials: cervical dysplasia Post Marketing Experience The following adverse reactions have been identified during post approval use of DRSP and EE. Because these reactions are reported voluntarily from a population of uncertain size, it is not always possible to reliably estimate their frequency or establish a causal relationship to drug exposure. Adverse reactions are grouped into System Organ Classes, and ordered by frequency. Vascular Disorders: Venous and arterial thromboembolic events (including pulmonary emboli, deep vein thrombosis, cerebral thrombosis, retinal thrombosis, myocardial infarction and stroke), hypertension (including hypertensive crisis) Hepatobiliary Disorders: Gallbladder disease, liver function disturbances, liver tumors Immune System Disorders: Hypersensitivity (including anaphylactic reaction) Metabolism and Nutrition Disorders: Hyperkalaemia, hypertriglyceridaemia, changes in glucose tolerance or effect on peripheral insulin resistance (including diabetes mellitus) Skin and Subcutaneous Tissue Disorders: Chloasma, angio-oedema, erythema nodosum, erythema multiforme Gastrointestinal Disorders: Inflammatory bowel disease Musculoskeletal and Connective Tissue Disorders: Systemic lupus erythematosus Overdosage There have been no reports of serious ill effects from overdose, including ingestion by children. Overdosage may cause withdrawal bleeding in females and nausea. DRSP is a spironolactone analogue having anti-mineralocorticoid properties. Serum concentration of potassium and sodium, and evidence of metabolic acidosis, should be monitored in cases of overdose. Storage And Handling Instructions Store in a cool, dry place.
Packaging Information CRISANTA-LS is available in a pack of 24 tablets. Last updated: December 2015 Last reviewed: December 2015 CRISANTA LS Tablets Source URL: https://ciplamed.com/content/crisanta-ls-tablets